首页> 外文期刊>Journal of physiology and pharmacology: an official journal of the Polish Physiological Society >ALTERATIONS IN THE LIVER OF INTRAUTERINE GROWTH RETARDED PIGLETS MAY PREDISPOSE TO DEVELOPMENT OF INSULIN RESISTANCE AND OBESITY IN LATER LIFE
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ALTERATIONS IN THE LIVER OF INTRAUTERINE GROWTH RETARDED PIGLETS MAY PREDISPOSE TO DEVELOPMENT OF INSULIN RESISTANCE AND OBESITY IN LATER LIFE

机译:宫内生长迟缓的仔猪肝脏的改变可能预示着其胰岛素抵抗和肥胖的发展

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Intrauterine growth retardation (IUGR) leads to increased predisposition to metabolic syndrome in adult life but the mechanisms remain obscure. Considering a significant number of functional similarities, IUGR piglets appear to be a good model to study the development of this syndrome in humans. The aim of the present study was to investigate the ultrastructure and proteomic profile of the liver in IUGR pig neonates to discover early markers of predisposition to obesity and insulin resistance. In our study intestine and liver tissue samples were investigated in 7 day old IUGR and normal body weight (NBW) littermate piglets using histometry, mass spectrometry, in-tissue cytometry analysis and confocal microscopy. Compared to NBW, the liver in IUGR neonates was characterized by a significantly enhanced ratio of Kupffer cells to hepatocytes and insulin receptor abundance as well as higher percentages of cells expressing receptors for adipokines (resistin and adiponectin), increased expression of TNF-α (as marker of inflammation), and increased expression of insulin receptor and uncoupling protein 3 (UCP3). Moreover, NBW and IUGR differed in proteomic profile, including protein metabolism (proteasomes, cathepsin D, phermitin, phosphoglucomutase), carbohydrate metabolism (hexokinase 1, phosphoglucokinase, galactokinase, aldolase B, glucose-6-phosphate isomerase), oxidative stress and chromatin organization and DNA uptake (histones, lamin a/c). Reduction of hepatocyte numbers concomitant with significant modifications of expression of key hormones and enzymes for protein and carbohydrate metabolism in IUGR neonates may predispose to insulin resistance and obesity in adult life.
机译:宫内发育迟缓(IUGR)导致成人代谢综合征的易感性增加,但机制仍不清楚。考虑到大量的功能相似性,IUGR仔猪似乎是研究该综合征在人类中发展的良好模型。本研究的目的是研究IUGR猪新生儿肝脏的超微结构和蛋白质组学特征,以发现肥胖和胰岛素抵抗易感性的早期标志物。在我们的研究中,使用组织学,质谱,组织内细胞计数法和共聚焦显微镜对7日龄IUGR和正常体重(NBW)同窝仔猪的肠和肝组织样本进行了调查。与NBW相比,IUGR新生儿的肝脏的特征是库普弗细胞与肝细胞和胰岛素受体丰度的比率显着提高,以及表达脂肪因子受体(抵抗素和脂联素)的细胞百分比更高,TNF-α的表达增加(如炎症标志物),并增加胰岛素受体和解偶联蛋白3(UCP3)的表达。此外,NBW和IUGR在蛋白质组学方面有所不同,包括蛋白质代谢(蛋白酶体,组织蛋白酶D,信息素,磷酸葡萄糖突变酶),碳水化合物代谢(己糖激酶1,磷酸葡萄糖激酶,半乳糖激酶,醛缩酶B,葡萄糖-6-磷酸异构酶),氧化应激和染色质组织和DNA摄取(组蛋白,层粘连蛋白a / c)。 IUGR新生儿中肝细胞数量的减少与关键激素和蛋白质和碳水化合物代谢关键酶表达的显着改变可能会导致成人胰岛素抵抗和肥胖。

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